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Properties and protective value of the secondary versus primary T helper type 1 response to airborne Mycobacterium tuberculosis infection in mice

机译:小鼠空中结核分枝杆菌感染继发性和主要性T辅助1型应答的特性和保护价值

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摘要

Mice immunized against Mycobacterium tuberculosis (Mtb) infection by curing them of a primary lung infection were compared with naive mice in terms of the ability to generate a Th1 cell immune response and to control growth of an airborne Mtb challenge infection. Immunized mice generated and expressed Th1 cell immunity several days sooner than naive mice, as demonstrated by an earlier increase in the synthesis in the lungs of mRNA for Th1 cytokines and for inducible nitric oxide synthase, an indicator of macrophage activation. This Th1 cytokine/mRNA synthesis was accompanied by an earlier accumulation of Mtb-specific Th1 cells in the lungs and the presence of CD4 T cells in lesions. An earlier generation of immunity was associated with an earlier inhibition of Mtb growth when infection was at a 1-log lower level. However, inhibition of Mtb growth in immunized, as well as in naive, mice was not followed by resolution of the infection, but by stabilization of the infection at a stationary level. The results indicate that there is no reason to believe that the secondary response to an Mtb infection is quantitatively or qualitatively superior to the primary response.
机译:将通过治愈原发性肺部感染而针对结核分枝杆菌(Mtb)感染免疫的小鼠与天真小鼠进行比较,以产生Th1细胞免疫反应和控制机载Mtb挑战性感染的生长的能力。免疫的小鼠比幼稚的小鼠快几天产生并表达Th1细胞免疫,这可以通过Th1细胞因子和可诱导的一氧化氮合酶(巨噬细胞激活的指示剂)的mRNA合成在肺中的增加来证明。这种Th1细胞因子/ mRNA的合成伴随着Mtb特异性Th1细胞在肺中的早期积累以及病变中CD4 T细胞的存在。当感染水平降低1个对数时,较早的免疫力与较早的Mtb生长抑制相关。但是,在免疫小鼠和幼稚小鼠中抑制Mtb的生长并不能解决感染,而是可以稳定地将感染稳定下来。结果表明,没有理由相信对Mtb感染的继发反应在数量上或质量上都优于原发反应。

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